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Triple-threat activity of PEDF in bone tumors: Tumor inhibition, tissue preservation and cardioprotection against doxorubicin

机译:骨肿瘤中PEDF的三威胁活动:肿瘤抑制,组织保存和对多柔比星的心脏保护

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Pigment epithelium-derived factor (PEDF) is known for its osteogenic properties, but its effects against primary and secondary bone tumors have not comprehensively been demonstrated. We show the ubiquitous expression of PEDF in murine embryonic tissue. Continuous administration of PEDF in pregnant mice for five days did not adversely affect foetal health, despite PEDF's known potent antiangiogenic properties. In the case of the devastating childhood bone cancer osteosarcoma, PEDF has direct anticancer activity per se, and protects against the toxicity of doxorubicin in the heart, small intestine and testes. PEDF demonstrated anti-proliferative and pro-apoptotic effects against human prostate and breast cancer cells, tumors which are known to metastasize to bone as the preferred secondary site. Caspase-2 was activated in both tumor cell types by PEDF. In models of prostate and breast cancer in bone, PEDF significantly reduced tumor volumes. When combined with zoledronic acid, continuously-administered PEDF significantly reduced breast tumor volume at the bone, and was able to preserve the quality of bone better than the combination therapy. These multiple positive findings make PEDF an ideal endogenous and safe biological for possible future clinical testing.
机译:颜料上皮衍生的因子(PEDF)以其成骨特性已知,但其对初级和继发性肿瘤的影响尚未综合地证明。我们展示了小鼠胚胎组织的PEDF的无处不在的表达。尽管PEDF已知的有效抗血管生成特性,但孕妇孕鼠的连续施用PEDF在孕鼠中的孕鼠持续5天。在毁灭性的儿童骨癌骨膜瘤的情况下,PEDF具有直接的抗癌活性本身,并防止对心脏,小肠和睾丸的多柔比星的毒性。 PEDF证明了针对人前列腺和乳腺癌细胞的抗增殖和促凋亡作用,已知将其作为优选的次级部位转移到骨的肿瘤。通过PEDF在肿瘤细胞类型中激活Caspase-2。在骨前列腺和乳腺癌模型中,PEDF显着减少了肿瘤体积。当与唑醇酸结合时,连续施用的PEDF在骨骼上显着降低乳腺肿瘤体积,并且能够比联合治疗更好地保持骨骼的质量。这些多个阳性发现使PEDF成为可能的未来临床测试的理想内源性和安全生物学。

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